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Structure of the hepatitis C virus IRES bound to the human 80S ribosome: Remodeling of the HCVIRES
被引:142
作者:

Boehringer, D
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机构: Max Planck Inst Biophys Chem, D-37077 Gottingen, Germany

Thermann, R
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机构: Max Planck Inst Biophys Chem, D-37077 Gottingen, Germany

Ostareck-Lederer, A
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机构: Max Planck Inst Biophys Chem, D-37077 Gottingen, Germany

Lewis, JD
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机构: Max Planck Inst Biophys Chem, D-37077 Gottingen, Germany

Stark, H
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机构: Max Planck Inst Biophys Chem, D-37077 Gottingen, Germany
机构:
[1] Max Planck Inst Biophys Chem, D-37077 Gottingen, Germany
[2] Anadys Pharmaceut, San Diego, CA 92121 USA
来源:
关键词:
D O I:
10.1016/j.str.2005.08.008
中图分类号:
Q5 [生物化学];
Q7 [分子生物学];
学科分类号:
071010 ;
081704 ;
摘要:
Initiation of translation of the hepatitis C virus (HCV) polyprotein is driven by an internal ribosome entry site (IRES) RNA that bypasses much of the eukaryotic translation initiation machinery. Here, single-particle electron cryomicroscopy has been used to study the mechanism of HCV IRES-mediated initiation. A HeLa in vitro translation system was used to assemble human IRES-80S ribosome complexes under near physiological conditions; these were stalled before elongation. Domain 2 of the HCV IRES is bound to the tRNA exit site, touching the L1 stalk of the 60S subunit, suggesting a mechanism for the removal of the HCV IRES in the progression to elongation. Domain 3 of the HCV IRES positions the initiation codon in the ribosomal mRNA binding cleft by binding helix 28 at the head of the 40S subunit. The comparison with the previously published binary 40S-HCV IRES complex reveals structural rearrangements in the two pseudoknot structures of the HCV IRES in translation initiation.
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页码:1695 / 1706
页数:12
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